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Controlling the kinetics of interferon transgene expression for improved gene therapy

机译:控制干扰素转基因表达的动力学以改善基因治疗

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Interferon (IFN) gene based therapy has been studied for the treatment of many diseases such as viral infections, cancer and allergic diseases. Non-viral vectors, like plasmid DNA, are promising ways for delivering IFN genes, because of their low immunogenicity and toxicity compared with viral vectors. Potent therapeutic effects of IFN gene transfer will depend on the level and duration of transgene expression after in vivo administration. Therefore, controlling the kinetics of transgene expression of IFNs is a rational approach for improved gene therapy. The design and optimization of plasmid vectors, as well as their route/method of administration, is the key to obtaining high and persistent transgene expression. In this review, we aim to present experimental evidence about the relationships among the properties of plasmid vectors expressing IFNs, the kinetics of transgene expression, and therapeutic effects as well as safety issues.
机译:已经研究了基于干扰素(IFN)基因的疗法来治疗许多疾病,例如病毒感染,癌症和过敏性疾病。非病毒载体,如质粒DNA,由于与病毒载体相比具有较低的免疫原性和毒性,因此是传递IFN基因的有前途的方法。 IFN基因转移的有效治疗效果将取决于体内给药后转基因表达的水平和持续时间。因此,控制IFNs转基因表达的动力学是改善基因治疗的合理方法。质粒载体的设计和优化及其给药途径/方法,是获得高水平和持久性转基因表达的关键。在这篇综述中,我们旨在提供有关表达IFN的质粒载体的性质,转基因表达的动力学,治疗效果以及安全性问题之间关系的实验证据。

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